Targeted NGS gene panel identifies mutations in RSPH1 causing primary ciliary dyskinesia and a common mechanism for ciliary central pair agenesis due to radial spoke defects

Onoufriadis, Alexandros; Shoemark, Amelia; Schmidts, Miriam; Patel, Mitali; Jimenez, Gina; Liu, Hui; Thomas, Biju; Dixon, Mellisa; Hirst, Robert A.; Rutman, A; Burgoyne, Thomas; Williams, Chris; Scully, Juliet; Bolard, Florence; Lafitte, Jean-Jacques; Beales, Philip L.; Hogg, Claire; Yang, Pinfen; Chung, Eddie M.K.; Emes, Richard D.; O’Callaghan, Christopher; K, Uk; Bouvagnet, Patrice; Mitchison, Hannah M.

doi:10.1093/hmg/ddu046

Cited by 76 publications

(76 citation statements)

References 54 publications

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“…PCD due to defects in RS function are very difficult to diagnose, because ultrastructural analyses of cross-sections studied by TEM can be normal (33)(34)(35)(36)(37)45), and some RS complexes can still be observed in TEM sections of patients with RSPH1 and RSPH4A mutations (35,36,46). Furthermore, ciliary beating abnormalities are very subtle and only detectable by experienced HSVM examiners (33,(35)(36)(37)45).…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, ciliary beating abnormalities are very subtle and only detectable by experienced HSVM examiners (33,(35)(36)(37)45). Here, we searched for mutations in RSPH9, RSPH4A, and RSPH1 in individuals with classical PCD symptoms with situs solitus, frequently normal TEM findings, and subtle changes in the ciliary beating pattern, as evaluated by HSVM (Table 1).…”

Section: Discussionmentioning

confidence: 99%

“…C, rs151107532; mutation of the obligatory canonical splice site; c.433C.T, p.Gln145* in RSPH1) have been reported previously (35)(36)(37)41). The mutation c.275-2A.C [p.?]…”

Section: Mutationalmentioning

confidence: 99%

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Immunofluorescence analysis and diagnosis of primary ciliary dyskinesia with radial spoke defects

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Frommer

Hjeij

et al. 2015

7.4 Paediatric Respiratory Infection and Immunology

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Primary ciliary dyskinesia (PCD) is a genetically heterogeneous recessive disorder caused by several distinct defects in genes responsible for ciliary beating, leading to defective mucociliary clearance often associated with randomization of left/right body asymmetry. Individuals with PCD caused by defective radial spoke (RS) heads are difficult to diagnose owing to lack of gross ultrastructural defects and absence of situs inversus. Thus far, most mutations identified in human radial spoke genes (RSPH) are loss-of-function mutations, and missense variants have been rarely described. We studied the consequences of different RSPH9, RSPH4A, and RSPH1 mutations on the assembly of the RS complex to improve diagnostics in PCD. We report 21 individuals with PCD (16 families) with biallelic mutations in RSPH9, RSPH4A, and RSPH1, including seven novel mutations comprising missense variants, and performed high-resolution immunofluorescence analysis of human respiratory cilia. Missense variants are frequent genetic defects in PCD with RS defects. Absence of RSPH4A due to mutations in RSPH4A results in deficient axonemal assembly of the RS head components RSPH1 and RSPH9. RSPH1 mutant cilia, lacking RSPH1, fail to assemble RSPH9, whereas RSPH9 mutations result in axonemal absence of RSPH9, but do not affect the assembly of the other head proteins, RSPH1 and RSPH4A. Interestingly, our results were identical in individuals carrying loss-of-function mutations, missense variants, or one amino acid deletion. Immunofluorescence analysis can improve diagnosis of PCD in patients with loss-of-function mutations as well as missense variants. RSPH4A is the core protein of the RS head.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Immunofluorescence analysis and diagnosis of primary ciliary dyskinesia with radial spoke defects

Loges

Frommer

Hjeij

et al. 2015

7.4 Paediatric Respiratory Infection and Immunology

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“…After purification, only the purified captured fragments are sequenced, allowing increased sequencing depth and thereby accuracy at a lower cost. This is the basis for the development of diagnostic disease-focused multigene panels Brett et al 2014;Lepri et al 2014;Onoufriadis et al 2014;Xue et al 2014), containing tens to up to hundreds of genes, as well as for WES (Lemke et al 2012;Korf 2013;Xue et al 2014). For WES, the baits are designed to capture the coding exons of nearly all genes, which represent 1% -2% of the total genomic DNA but contain 85% of known disease causing mutations (Bick and Dimmock 2011;Gilissen et al 2012;Gonzaga-Jauregui et al 2012;Korf and Rehm 2013;Xue et al 2014).…”

Section: Next-generation Sequencing (Ngs) Technology and Pitfallsmentioning

confidence: 99%

“…Rather than a lengthy stepwise approach with sequential mutation analysis of the most obvious candidate genes first, followed by analysis of less-likely candidate genes, disease-focused NGS panels permit analysis of up to several hundreds of genes at once for defined categories of phenotypes, such as congenital heart defects, skeletal dysplasias, mitochondrial disorders, disorders of glycosylation, ciliopathies, cardiac defects, epilepsies, Noonan syndrome, etc. Korf 2013;Valencia et al 2013;Brett et al 2014;Chen et al 2014;Lepri et al 2014;Onoufriadis et al 2014;Xue et al 2014).…”

Section: Applications Of Diagnostic Sequencing In the Adult And Pediamentioning

confidence: 99%

Genome-Wide Sequencing for Prenatal Detection of Fetal Single-Gene Disorders

Veyver

Eng

2015

Cold Spring Harb Perspect Med

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Mammalian axoneme central pair complex proteins: Broader roles revealed by gene knockout phenotypes

et al. 2016

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The axoneme genes, their encoded proteins, their functions and the structures they form are largely conserved across species. Much of our knowledge of the function and structure of axoneme proteins in cilia and flagella is derived from studies on model organisms like the green algae, Chlamydomonas reinhardtii. The core structure of cilia and flagella is the axoneme, which in most motile cilia and flagella contains a 9 + 2 configuration of microtubules. The two central microtubules are the scaffold of the central pair complex (CPC). Mutations that disrupt CPC genes in Chlamydomonas and other model organisms result in defects in assembly, stability and function of the axoneme, leading to flagellar motility defects. However, targeted mutations generated in mice in the orthologous CPC genes have revealed significant differences in phenotypes of mutants compared to Chlamydomonas. Here we review observations that support the concept of cell-type specific roles for the CPC genes in mice, and an expanded repertoire of functions for the products of these genes in cilia, including non-motile cilia, and other microtubule-associated cellular functions.

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Targeted NGS gene panel identifies mutations in RSPH1 causing primary ciliary dyskinesia and a common mechanism for ciliary central pair agenesis due to radial spoke defects

Cited by 76 publications

References 54 publications

Immunofluorescence analysis and diagnosis of primary ciliary dyskinesia with radial spoke defects

Immunofluorescence analysis and diagnosis of primary ciliary dyskinesia with radial spoke defects

Genome-Wide Sequencing for Prenatal Detection of Fetal Single-Gene Disorders

Mammalian axoneme central pair complex proteins: Broader roles revealed by gene knockout phenotypes

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